Literature DB >> 16687622

Functional GABA(A)-receptor-mediated inhibition in the neonatal dorsal horn.

L Bremner1, M Fitzgerald, M Baccei.   

Abstract

Neonatal nociceptive circuits and dorsal horn cells are characterized by an apparent lack of inhibitory control: receptive fields are large and thresholds low in the first weeks of life. It has been suggested that this may reflect immature GABA(A)-receptor (GABA(A)R) signaling whereby an early developmental shift in transmembrane anion gradient is followed by a longer period of low Cl- extrusion capacity. To investigate whether functional GABA(A)R-mediated inhibition does indeed undergo postnatal regulation at the level of dorsal horn circuits, we applied the selective GABA(A)R antagonist gabazine to the spinal cord in anesthetized rat pups [postnatal day (P) 3 or 21] while recording spike activity in single lumbar dorsal horn cells in vivo. At both ages, blockade of GABA(A)R activity resulted in enlarged hind paw receptive field areas and increased activity evoked by low- and high-intensity cutaneous stimulation, revealing comparable inhibition of dorsal horn cell firing by spinal GABA(A)Rs at P3 and P21. This inhibition did not require descending pathways to the spinal cord because perforated patch-clamp recordings of deep dorsal horn neurons in P3 spinal cord slices also showed an increase in evoked spike activity after application of gabazine. We conclude that spinal GABAergic inhibitory transmission onto single dorsal horn cells "in vivo" is functional at P3 and that low Cl- extrusion capacity does not restrict GABAergic function over the normal range of evoked sensory activity. The excitability of neonatal spinal sensory circuits could reflect immaturity in other intrinsic or descending inhibitory networks rather than weak spinal GABAergic inhibition.

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Year:  2006        PMID: 16687622     DOI: 10.1152/jn.00123.2006

Source DB:  PubMed          Journal:  J Neurophysiol        ISSN: 0022-3077            Impact factor:   2.714


  10 in total

1.  C-fiber activity-dependent maturation of glycinergic inhibition in the spinal dorsal horn of the postnatal rat.

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2.  Detection of submillisecond spike timing differences based on delay-line anticoincidence detection.

Authors:  Ariel M Lyons-Warren; Tsunehiko Kohashi; Steven Mennerick; Bruce A Carlson
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Review 3.  The development of pain circuits and unique effects of neonatal injury.

Authors:  Chelsie L Brewer; Mark L Baccei
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4.  Postnatal tuning of cutaneous inhibitory receptive fields in the rat.

Authors:  Lindsay R Bremner; Maria Fitzgerald
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Review 5.  Neuraxial analgesia in neonates and infants: a review of clinical and preclinical strategies for the development of safety and efficacy data.

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6.  Neonatal tissue injury reduces the intrinsic excitability of adult mouse superficial dorsal horn neurons.

Authors:  J Li; M L Baccei
Journal:  Neuroscience       Date:  2013-11-01       Impact factor: 3.590

Review 7.  Fast synaptic inhibition in spinal sensory processing and pain control.

Authors:  Hanns Ulrich Zeilhofer; Hendrik Wildner; Gonzalo E Yévenes
Journal:  Physiol Rev       Date:  2012-01       Impact factor: 37.312

8.  Postnatal maturation of spinal dynorphin circuits and their role in somatosensation.

Authors:  Chelsie L Brewer; Lauren M Styczynski; Elizabeth K Serafin; Mark L Baccei
Journal:  Pain       Date:  2020-08       Impact factor: 7.926

9.  Transient, activity dependent inhibition of transmitter release from low threshold afferents mediated by GABAA receptors in spinal cord lamina III/IV.

Authors:  Chiara Betelli; Amy B MacDermott; Rita Bardoni
Journal:  Mol Pain       Date:  2015-10-13       Impact factor: 3.395

Review 10.  Early Neonatal Pain-A Review of Clinical and Experimental Implications on Painful Conditions Later in Life.

Authors:  Morika D Williams; B Duncan X Lascelles
Journal:  Front Pediatr       Date:  2020-02-07       Impact factor: 3.418

  10 in total

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